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Calcifications in human osteoarthritic articular cartilage: Ex vivo assessment of calcium compounds using XANES spectroscopy

机译:人骨关节炎关节钙化:使用XANES光谱的钙化合物的离体评估

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Calcium (Ca~(2+))-containing crystals (CCs), including basic Ca~(2+) phosphate (BCP) and Ca~(2+) pyrophosphate dihydrate (CPPD) crystals, are associated with severe forms of osteoarthritis (OA). Growing evidence supports a role for abnormal articular cartilage mineralization in the pathogenesis of OA. However, the role of Ca~(2+) compounds in this mineralization process remains poorly understood. Six patients, who underwent total knee joint replacement for primary OA, have been considered in this study. Cartilage from femoral condyles and tibial plateaus in the medial and lateral compartments was collected as 1 mm-thick slices cut tangentially to the articular surface. First, CCs presence and biochemical composition were assessed using Fourier transform infrared spectroscopy (FT-IR). Next, Ca ~(2+) compound biochemical form was further assessed using X-ray absorption spectroscopy (XAS) performed at the Ca~(2+) K-absorption edge. Overall, 12 cartilage samples were assessed. Using FT-IR, BCP and CPPD crystals were detected in four and three out of 12 samples, respectively. Ca~(2+) compound biochemical forms differed between areas with versus without CCs, when compared using XAS. The complete set of data shows that XANES spectroscopy can be used to accurately characterize sparse CCs in human OA cartilage. It is found that Ca~(2+) compounds differ between calcified and non-calcified cartilage areas. In calcified areas they appear to be mainly involved in calcifications, namely Ca~(2+) crystals.
机译:含钙(Ca〜(2+))的晶体(CC),包括碱性磷酸Ca〜(2+)(BCP)和焦磷酸Ca〜(2+)二水合物(CPPD)晶体,与严重的骨关​​节炎有关( OA)。越来越多的证据支持异常关节软骨矿化在OA发病机理中的作用。然而,Ca〜(2+)化合物在该矿化过程中的作用仍然知之甚少。本研究考虑了六例接受全膝关节置换以治疗原发性OA的患者。取自内侧和外侧隔室的股骨dy和胫骨平台的软骨,将其切成与关节表面相切的1毫米厚的切片。首先,使用傅里叶变换红外光谱(FT-IR)评估CC的存在和生化成分。接下来,使用在Ca〜(2+)K吸收边缘进行的X射线吸收光谱(XAS)进一步评估Ca〜(2+)化合物的生化形式。总体上,评估了12个软骨样品。使用FT-IR,分别在12个样品中的4个和3个中检测到BCP和CPPD晶体。使用XAS进行比较时,含CC和不含CC的区域之间的Ca〜(2+)化合物生化形式有所不同。完整的数据集表明,XANES光谱可用于准确表征人OA软骨中的稀疏CC。发现钙〜和非钙软骨区域之间的Ca〜(2+)化合物不同。在钙化区域,它们似乎主要参与钙化,即Ca〜(2+)晶体。

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